Epoxyalcohols: Bioactivation and Conjugation Required for Skin Sensitization
详细信息 查看全文
- 作者:Tamara Delaine ; David J. Ponting ; Ida B. Niklasson ; Roger Emter ; Lina Hagvall ; Per-Ola Norrby ; Andreas Natsch ; Kristina Luthman ; Ann-Therese Karlberg
- 刊名:Chemical Research in Toxicology
- 出版年:2014
- 出版时间:October 20, 2014
- 年:2014
- 卷:27
- 期:10
- 页码:1860-1870
- 全文大小:439K
- ISSN:1520-5010
文摘
Allylic alcohols, such as geraniol 1, are easily oxidized by varying mechanisms, including the formation of both 2,3-epoxides and/or aldehydes. These epoxides, aldehydes, and epoxy-aldehydes can be interconverted to each other, and the reactivity of them all must be considered when considering the sensitization potential of the parent allylic alcohol. An in-depth study of the possible metabolites and autoxidation products of allylic alcohols is described, covering the formation, interconversion, reactivity, and sensitizing potential thereof, using a combination of in vivo, in vitro, in chemico, and in silico methods. This multimodal study, using the integration of diverse techniques to investigate the sensitization potential of a molecule, allows the identification of potential candidate(s) for the true culprit(s) in allergic responses to allylic alcohols. Overall, the sensitization potential of the investigated epoxyalcohols and unsaturated alcohols was found to derive from metabolic oxidation to the more potent aldehyde where possible. Where this is less likely, the compound remains weakly or nonsensitizing. Metabolic activation of a double bond to form a nonconjugated, nonterminal epoxide moiety is not enough to turn a nonsensitizing alcohol into a sensitizer, as such epoxides have low reactivity and low sensitizing potency. In addition, even an allylic 2,3-epoxide moiety is not necessarily a potent sensitizer, as shown for 2, where formation of the epoxide weakens the sensitization potential.